Doxapram (Monograph)
Brand name: Dopram
Drug class: Respiratory and CNS Stimulants
VA class: RE900
CAS number: 7081-53-0
Introduction
CNS stimulant; a monohydrated pyrrolidinone derivative.
Uses for Doxapram
Postanesthetic Respiratory Depression
Treatment of drug-induced postanesthetic respiratory depression or apnea not caused by skeletal muscle relaxants.
Other supportive therapy preferred due to questionable benefit and high potential for toxicity with doxapram. Limited role due to availability of safer and shorter-acting anesthetic agents.
Drug-induced CNS Depression
Has been used in conjunction with supportive measures to stimulate respiration and hasten arousal in patients with respiratory and CNS depression secondary to drug overdose (e.g., barbiturates, opiate analgesics, general anesthetics).
However, use as an analeptic is strongly discouraged by most clinicians; analeptic therapy largely abandoned in favor of intensive supportive care (e.g., mechanical ventilation, oxygenation, cardiovascular support) and specific antidotes (e.g., pure opiate antagonists).
Acute Hypercapnia Associated with COPD
Short-term use in patients with acute respiratory insufficiency associated with COPD.
Role in such patients is limited; other supportive therapy (i.e., noninvasive ventilation using either negative- or positive-pressure device) is preferred.
Neonatal Apnea
Has been used for the treatment of neonatal apnea† [off-label], principally in combination with theophylline or caffeine.
Limited support for this use; no apparent advantage over methylxanthines and risk of substantial adverse effects with doxapram therapy. The commercially available injection contains benzyl alcohol; use of this preparation in neonates is not recommended. (See Pediatric Use under Cautions.)
Other Uses
Should not be used in conjunction with mechanical ventilation.
Doxapram Dosage and Administration
General
-
Establish adequate airway and oxygenation prior to administration; take measures to prevent vomiting and aspiration.
-
Use minimum effective dosage to avoid adverse effects.
-
Monitor BP, heart rate, and deep tendon reflexes; adjust dosage or rate of infusion accordingly. Monitor for recurrence of unconsciousness or development of respiratory depression; provide supportive care as required.
Administration
IV Administration
For solution and drug compatibility information, see Compatibility under Stability.
Administer by IV injection or IV infusion.
Predictable blood gas patterns in patients with COPD and acute hypercapnia are more readily established with IV infusion therapy.
Avoid extravasation and repeated use of a single injection site to minimize local reactions and thrombophlebitis.
Dilution
Prepare 1-mg/mL solution by adding 250 mg of doxapram hydrochloride (12.5 mL) to 250 mL of 5% dextrose, 10% dextrose, or 0.9% sodium chloride injection.
Prepare 2-mg/mL solution by adding 400 mg of doxapram hydrochloride (20 mL) to 180 mL of 5% dextrose, 10% dextrose, or 0.9% sodium chloride injection.
Rate of Administration
Rapid infusion may result in hemolysis; infuse diluted solution at slow rate.
Postanesthetic use: Initiate IV infusion with 1-mg/mL solution at a rate of approximately 5 mg/minute until desired response achieved; usual maintenance rate is 1–3 mg/minute.
Acute hypercapnia associated with COPD: Initiate IV infusion with 2-mg/mL solution at a rate of 1–2 mg/minute; may increase to maximum rate of 3 mg/minute.
Dosage
Available as doxapram hydrochloride; dosage expressed in terms of the salt.
Pediatric Patients
Postanesthetic Respiratory Depression
IV Injection
Children ≥12 years of age: 0.5–1 mg/kg as a single injection; may repeat every 5 minutes to a maximum total dosage of 2 mg/kg.
IV Infusion
Children ≥12 years of age: 0.5–1 mg/kg, up to a maximum dosage of 4 mg/kg.
Acute Hypercapnia Associated with COPD
IV Infusion
Children ≥12 years of age: Initiate at a rate of 1–2 mg/minute; increase to a maximum rate of 3 mg/minute if indicated. Continuation beyond a single 2-hour infusion not recommended.
Adults
Postanesthetic Respiratory Depression
IV Injection
0.5–1 mg/kg as a single injection; may repeat every 5 minutes to a maximum total dosage of 2 mg/kg.
IV Infusion
0.5–1 mg/kg, up to a maximum dosage of 4 mg/kg.
Acute Hypercapnia Associated with COPD
IV Infusion
Initiate at a rate of 1–2 mg/minute; increase to a maximum rate of 3 mg/minute if indicated. Continuation beyond a single 2-hour infusion not recommended.
Prescribing Limits
Pediatric Patients
Postanesthetic Respiratory Depression
IV Injection
Children ≥12 years of age: Maximum 1.5 mg/kg for a single injection, 2-mg/kg total dosage for repeat injections; do not exceed 3 g daily.
IV Infusion
Children ≥12 years of age: Maximum 4 mg/kg; do not exceed 3 g daily.
Acute Hypercapnia Associated with COPD
IV Infusion
Children ≥12 years of age: Maximum 3 mg/minute. Limit use to a single 2-hour infusion.
Adults
Postanesthetic Respiratory Depression
IV Injection
Maximum 1.5 mg/kg for a single injection, 2-mg/kg total dosage for repeat injections; do not exceed 3 g daily.
IV Infusion
Maximum 4 mg/kg; do not exceed 3 g daily.
Acute Hypercapnia Associated with COPD
IV Infusion
Maximum 3 mg/minute. Limit use to a single 2-hour infusion.
Special Populations
No special population dosage recommendations at this time.
Cautions for Doxapram
Contraindications
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Known hypersensitivity to doxapram or any ingredient in the formulation.
-
Seizure disorders.
-
Suspected or confirmed pulmonary embolism.
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Mechanical disorders of ventilation (e.g., mechanical obstruction, muscle paresis, flail chest, pneumothorax, acute bronchial asthma, pulmonary fibrosis or other restrictive lung diseases).
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Head injury, cerebrovascular accident, or cerebral edema.
-
Substantial cardiovascular impairment (i.e., uncompensated heart failure, severe CAD).
-
Severe hypertension including that associated with hyperthyroidism or pheochromocytoma. (See Postanesthetic Use under Cautions.)
Warnings/Precautions
Warnings
Benzyl Alcohol in Neonates
Doxapram hydrochloride injection contains benzyl alcohol as a preservative, which has been associated with toxicity (including deaths) in neonates. Use of this preparation in neonates is not recommended. (See Pediatric Use under Cautions.)
Mechanical Ventilation
Do notuse doxapram in conjunction with mechanical ventilation.
Postanesthetic Use
Doxapram is not an antagonist to muscle relaxants nor a specific opiate antagonist. Assess adequacy of ventilation with specific tests (e.g., peripheral nerve stimulation, airway pressures, head lift, pulse oximetry, end-tidal carbon dioxide) prior to use.
Narcosis may recur; observe patient closely until fully alert for 0.5–1 hour.
Concomitant use with a volatile general anesthetic may increase potential for arrhythmias. (See Specific Drugs under Interactions.)
Use with caution in patients with hypermetabolic states (e.g., hyperthyroidism, pheochromocytoma).
Drug-Induced CNS and Respiratory Depression
May not be effective in patients with severe CNS or respiratory depression; manufacturers state that doxapram may be used adjunctively with established supportive and resuscitative measures.
If no response, perform neurologic evaluation to identify other potential causes of sustained coma.
COPD
Do not increase rate of infusion to lower carbon dioxide tension.
Arrhythmias have been reported in patients with acute respiratory failure secondary to COPD. Use with caution in these patients.
To prevent respiratory acidosis in patients with COPD, monitor arterial blood gases at baseline and every 30 minutes. Discontinue drug and initiate mechanical ventilation if arterial blood gases deteriorate.
Use does not reduce need for supplemental oxygen.
General Precautions
Cardiovascular Effects
Possible changes in heart rate, lowered T-waves, and dysrhythmias (e.g., ventricular tachycardia, ventricular fibrillation, QT interval prolongation). Use with caution and monitor cardiac rhythm.
Increases in BP usually are modest, but substantial increases reported. Avoid use in patients with severe hypertension. (See Contraindications under Cautions.)
Chest pain and tightness in chest also reported.
Discontinue drug if sudden hypotension develops.
Respiratory Effects
Establish and protect airways.
Discontinue drug if sudden dyspnea develops.
Lowered carbon dioxide tension induced by hyperventilation may cause cerebral vasoconstriction and decreased cerebral circulation. Pressor effect on pulmonary circulation may lead to decreased arterial oxygen tension. Monitor arterial blood gases.
CNS Effects
May cause seizures and other adverse effects due to general CNS stimulation. Anticonvulsants, oxygen, and resuscitative equipment should be readily available; carefully observe patient and administer drug slowly if treatment continued.
Local Effects
Potential for local reactions including thrombophlebitis; administer dilute solutions at a slow rate, prevent extravasation, and avoid repeated use of a single injection site.
Hemolysis
Rapid infusion may result in hemolysis. (See Rate of Administration under Dosage and Administration.)
Specific Populations
Pregnancy
Category B.
Lactation
Not known whether doxapram is distributed into milk; however, molecular weight of free base suggests drug may be distributed into milk.
Benzyl alcohol in commercial preparation is associated with toxicity in neonates; caution if used in nursing women. (See Pediatric Use under Cautions.)
Pediatric Use
Safety and efficacy not established in children <12 years of age.
Each mL of doxapram hydrochloride injection contains 9 mg of benzyl alcohol; use of this preparation in neonates is not recommended. Although a causal relationship has not been established, large amounts of benzyl alcohol (100–400 mg/kg daily) have been associated with toxicity in neonates.
Hepatic Impairment
Use with caution. Possible decrease in rate of metabolism or clearance in patients with substantial hepatic impairment.
Renal Impairment
Use with caution. Possible decrease in rate of metabolism or clearance in patients with substantial renal impairment.
Common Adverse Effects
Cough, dyspnea, tachypnea, headache, dizziness, apprehension, hypertension, flushing, sweating, nausea, vomiting, diarrhea, urinary retention, muscle spasticity.
Drug Interactions
Specific Drugs
|
Drug |
Interaction |
Comments |
|---|---|---|
|
Anesthetics, inhalation (known to sensitize myocardium to catecholamines) |
May increase potential for arrhythmias including ventricular tachycardia and ventricular fibrillation Increased BUN and albuminuria observed |
Delay administration of doxapram until anesthetic excreted Importance of observed increase in BUN and albuminuria not established |
|
CNS depressants |
Increased BUN and albuminuria observed |
Importance not established |
|
MAO inhibitors |
Possible synergistic pressor effect |
Use with caution |
|
Neuromuscular blocking agents |
May temporarily mask residual effects of muscle relaxants |
Use with caution |
|
Sympathomimetic agents |
Possible synergistic pressor effect |
Use with caution |
|
Theophyllines (e.g., aminophylline) |
Possible increased skeletal muscle activity, agitation, and hyperactivity |
Doxapram Pharmacokinetics
Absorption
Onset
Following single IV injection, onset of respiratory stimulation occurs within 20–40 seconds and peaks at 1–2 minutes.
Duration
Duration of respiratory stimulation may vary from 5–12 minutes following single IV injection.
Distribution
Extent
Doxapram and its metabolites are generally well distributed into tissues in animals.
Elimination
Metabolism
Rapidly metabolized following single IV dose. Undergoes hydroxylation to ketodoxapram, an active metabolite.
Elimination Route
Excreted mainly in urine and feces as metabolites within 24–48 hours following administration; following single IV dose, 40–50% of dose recovered in urine as metabolites; small amounts of metabolites may continue to be excreted for up to 120 hours.
Half-life
Elimination half-life approximately 6.6–9.9 hours in premature neonates receiving IV infusions of doxapram.
Stability
Storage
Parenteral
Injection
20–25°C.
Compatibility
Parenteral
Incompatible with strongly alkaline drugs or solutions.
Solution Compatibility127 137
|
Compatible |
|---|
|
Dextrose 5 or 10% in water |
|
Sodium chloride 0.9% |
Drug Compatibility
|
Incompatible |
|---|
|
Aminophylline |
|
Furosemide |
|
Sodium bicarbonate |
|
Thiopental sodium |
|
Ticarcillin |
|
Compatible |
|---|
|
Ampicillin sodium |
|
Caffeine citrate |
|
Calcium chloride |
|
Calcium gluconate |
|
Cefazolin sodium |
|
Ceftazidime |
|
Erythromycin lactobionate |
|
Fentanyl citrate |
|
Gentamicin sulfate |
|
Heparin sodium |
|
Metoclopramide HCl |
|
Metronidazole |
|
Oxacillin sodium |
|
Phenobarbital sodium |
|
Ranitidine HCl |
|
Vancomycin HCl |
|
Incompatible |
|
Clindamycin phosphate |
|
Compatible |
|---|
|
Amikacin sulfate |
|
Bumetanide |
|
Chlorpromazine HCl |
|
Cimetidine HCl |
|
Cisplatin |
|
Cyclophosphamide |
|
Dopamine HCl |
|
Doxycycline hyclate |
|
Epinephrine HCl |
|
Hydroxyzine HCl |
|
Isoniazid |
|
Lincomycin HCl |
|
Methotrexate sodium |
|
Phytonadione |
|
Pyridoxine HCl |
|
Terbutaline sulfate |
|
Thiamine HCl |
|
Tobramycin sulfate |
|
Vincristine sulfate |
|
Incompatible |
|
Aminophylline |
|
Ascorbic acid injection |
|
Cefotaxime |
|
Cefuroxime sodium |
|
Dexamethasone sodium phosphate |
|
Diazepam |
|
Digoxin |
|
Dobutamine HCl |
|
Folic acid |
|
Furosemide |
|
Hydrocortisone sodium phosphate |
|
Hydrocortisone sodium succinate |
|
Ketamine HCl |
|
Methylprednisolone sodium succinate |
|
Thiopental sodium |
Actions
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Stimulates peripheral carotid and aortic chemoreceptors and central respiratory centers in a dose-related manner. May cause tonic-clonic seizures with excessive CNS stimulation.
-
Transiently increases tidal volume with slight increase in respiratory rate.
-
May elicit a pressor response due to improved cardiac output and increased release of catecholamines. No direct effect on peripheral blood vessels.
-
Does not antagonize the analgesic effects of opiates.
Advice to Patients
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Importance of informing clinicians of existing or contemplated concomitant therapy, including prescription and OTC drugs, as well as any concomitant illnesses (e.g., cardiovascular disease, seizure disorders).
-
Importance of women informing their clinician if they are or plan to become pregnant or plan to breast-feed.
-
Importance of informing patients of other important precautionary information. (See Cautions.)
Preparations
Excipients in commercially available drug preparations may have clinically important effects in some individuals; consult specific product labeling for details.
Please refer to the ASHP Drug Shortages Resource Center for information on shortages of one or more of these preparations.
* available from one or more manufacturer, distributor, and/or repackager by generic (nonproprietary) name
|
Routes |
Dosage Forms |
Strengths |
Brand Names |
Manufacturer |
|---|---|---|---|---|
|
Parenteral |
Injection |
20 mg/mL* |
Dopram (with benzyl alcohol 0.9%) |
Baxter |
|
Doxapram Hydrochloride Injection (with benzyl alcohol 0.9%) |
Bedford |
AHFS DI Essentials™. © Copyright 2024, Selected Revisions November 20, 2012. American Society of Health-System Pharmacists, Inc., 4500 East-West Highway, Suite 900, Bethesda, Maryland 20814.
† Off-label: Use is not currently included in the labeling approved by the US Food and Drug Administration.
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